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一种关于癌症起源的新理论:量子相干纠缠、中心粒、有丝分裂与分化。

A new theory of the origin of cancer: quantum coherent entanglement, centrioles, mitosis, and differentiation.

作者信息

Hameroff Stuart R

机构信息

Department of Anesthesiology, and Center for Consciousness Studies, The University of Arizona, Tucson, AZ, USA.

出版信息

Biosystems. 2004 Nov;77(1-3):119-36. doi: 10.1016/j.biosystems.2004.04.006.

Abstract

Malignant cells are characterized by abnormal segregation of chromosomes during mitosis ("aneuploidy"), generally considered a result of malignancy originating in genetic mutations. However, recent evidence supports a century-old concept that maldistribution of chromosomes (and resultant genomic instability) due to abnormalities in mitosis itself is the primary cause of malignancy rather than a mere byproduct. In normal mitosis chromosomes replicate into sister chromatids which are then precisely separated and transported into mirror-like sets by structural protein assemblies called mitotic spindles and centrioles, both composed of microtubules. The elegant yet poorly understood ballet-like movements and geometric organization occurring in mitosis have suggested guidance by some type of organizing field, however neither electromagnetic nor chemical gradient fields have been demonstrated or shown to be sufficient. It is proposed here that normal mirror-like mitosis is organized by quantum coherence and quantum entanglement among microtubule-based centrioles and mitotic spindles which ensure precise, complementary duplication of daughter cell genomes and recognition of daughter cell boundaries. Evidence and theory supporting organized quantum states in cytoplasm/nucleoplasm (and quantum optical properties of centrioles in particular) at physiological temperature are presented. Impairment of quantum coherence and/or entanglement among microtubule-based mitotic spindles and centrioles can result in abnormal distribution of chromosomes, abnormal differentiation and uncontrolled growth, and account for all aspects of malignancy. New approaches to cancer therapy and stem cell production are suggested via non-thermal laser-mediated effects aimed at quantum optical states of centrioles.

摘要

恶性细胞的特征是在有丝分裂过程中染色体分离异常(“非整倍体”),通常认为这是源自基因突变的恶性肿瘤的结果。然而,最近的证据支持了一个百年前的概念,即由于有丝分裂本身的异常导致染色体分布不均(以及由此产生的基因组不稳定)是恶性肿瘤的主要原因,而不仅仅是一个副产品。在正常的有丝分裂中,染色体复制成姐妹染色单体,然后由称为有丝分裂纺锤体和中心粒的结构蛋白组件精确分离并运输到镜像般的两组中,这两者均由微管组成。有丝分裂中发生的优雅却鲜为人知的类似芭蕾舞的运动和几何组织表明存在某种类型的组织场的引导,然而,既没有证明电磁场也没有证明化学梯度场,也没有表明它们是足够的。本文提出,正常的镜像有丝分裂是由基于微管的中心粒和有丝分裂纺锤体之间的量子相干和量子纠缠组织起来的,这确保了子细胞基因组的精确、互补复制以及子细胞边界的识别。文中给出了支持生理温度下细胞质/核质中有序量子态(特别是中心粒的量子光学性质)的证据和理论。基于微管的有丝分裂纺锤体和中心粒之间的量子相干和/或纠缠受损会导致染色体分布异常、分化异常和生长失控,并解释了恶性肿瘤的所有方面。通过针对中心粒量子光学状态的非热激光介导效应,提出了癌症治疗和干细胞生产的新方法。

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